Deep serological profiling of the Trypanosoma cruzi TSSA antigen reveals different epitopes and modes of recognition by Chagas disease patients

BACKGROUND: Trypanosoma cruzi, the agent of Chagas disease, displays a highly structured population, with multiple strains that can be grouped into 6–7 evolutionary lineages showing variable eco-epidemiological traits and likely also distinct disease-associated features. Previous works have shown th...

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Autores principales: Romer, Guadalupe, Bracco, Leonel A., Ricci, Alejandro D., Balouz, Virginia, Berná, Luisa, Villar, Juan C., Ramsey, Janine M., Nolan, Melissa S., Torrico, Faustino, Kesper, Norival, Altcheh, Jaime, Robello, Carlos, Buscaglia, Carlos A., Agüero, Fernán
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2023
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10441789/
https://www.ncbi.nlm.nih.gov/pubmed/37556493
http://dx.doi.org/10.1371/journal.pntd.0011542
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author Romer, Guadalupe
Bracco, Leonel A.
Ricci, Alejandro D.
Balouz, Virginia
Berná, Luisa
Villar, Juan C.
Ramsey, Janine M.
Nolan, Melissa S.
Torrico, Faustino
Kesper, Norival
Altcheh, Jaime
Robello, Carlos
Buscaglia, Carlos A.
Agüero, Fernán
author_facet Romer, Guadalupe
Bracco, Leonel A.
Ricci, Alejandro D.
Balouz, Virginia
Berná, Luisa
Villar, Juan C.
Ramsey, Janine M.
Nolan, Melissa S.
Torrico, Faustino
Kesper, Norival
Altcheh, Jaime
Robello, Carlos
Buscaglia, Carlos A.
Agüero, Fernán
author_sort Romer, Guadalupe
collection PubMed
description BACKGROUND: Trypanosoma cruzi, the agent of Chagas disease, displays a highly structured population, with multiple strains that can be grouped into 6–7 evolutionary lineages showing variable eco-epidemiological traits and likely also distinct disease-associated features. Previous works have shown that antibody responses to ‘isoforms’ of the polymorphic parasite antigen TSSA enable robust and sensitive identification of the infecting strain with near lineage-level resolution. To optimize the serotyping performance of this molecule, we herein used a combination of immunosignaturing approaches based on peptide microarrays and serum samples from Chagas disease patients to establish a deep linear B-cell epitope profiling of TSSA. METHODS/PRINCIPLE FINDINGS: Our assays revealed variations in the seroprevalence of TSSA isoforms among Chagas disease populations from different settings, hence strongly supporting the differential distribution of parasite lineages in domestic cycles across the Americas. Alanine scanning mutagenesis and the use of peptides of different lengths allowed us to identify key residues involved in antibody pairing and the presence of three discrete B-cell linear epitopes in TSSAII, the isoform with highest seroprevalence in human infections. Comprehensive screening of parasite genomic repositories led to the discovery of 9 novel T. cruzi TSSA variants and one TSSA sequence from the phylogenetically related bat parasite T. cruzi marinkellei. Further residue permutation analyses enabled the identification of diagnostically relevant or non-relevant substitutions among TSSA natural polymorphisms. Interestingly, T. cruzi marinkellei TSSA displayed specific serorecognition by one chronic Chagas disease patient from Colombia, which warrant further investigations on the diagnostic impact of such atypical TSSA. CONCLUSIONS/SIGNIFICANCE: Overall, our findings shed new light into TSSA evolution, epitope landscape and modes of recognition by Chagas disease patients; and have practical implications for the design and/or evaluation of T. cruzi serotyping strategies.
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spelling pubmed-104417892023-08-22 Deep serological profiling of the Trypanosoma cruzi TSSA antigen reveals different epitopes and modes of recognition by Chagas disease patients Romer, Guadalupe Bracco, Leonel A. Ricci, Alejandro D. Balouz, Virginia Berná, Luisa Villar, Juan C. Ramsey, Janine M. Nolan, Melissa S. Torrico, Faustino Kesper, Norival Altcheh, Jaime Robello, Carlos Buscaglia, Carlos A. Agüero, Fernán PLoS Negl Trop Dis Research Article BACKGROUND: Trypanosoma cruzi, the agent of Chagas disease, displays a highly structured population, with multiple strains that can be grouped into 6–7 evolutionary lineages showing variable eco-epidemiological traits and likely also distinct disease-associated features. Previous works have shown that antibody responses to ‘isoforms’ of the polymorphic parasite antigen TSSA enable robust and sensitive identification of the infecting strain with near lineage-level resolution. To optimize the serotyping performance of this molecule, we herein used a combination of immunosignaturing approaches based on peptide microarrays and serum samples from Chagas disease patients to establish a deep linear B-cell epitope profiling of TSSA. METHODS/PRINCIPLE FINDINGS: Our assays revealed variations in the seroprevalence of TSSA isoforms among Chagas disease populations from different settings, hence strongly supporting the differential distribution of parasite lineages in domestic cycles across the Americas. Alanine scanning mutagenesis and the use of peptides of different lengths allowed us to identify key residues involved in antibody pairing and the presence of three discrete B-cell linear epitopes in TSSAII, the isoform with highest seroprevalence in human infections. Comprehensive screening of parasite genomic repositories led to the discovery of 9 novel T. cruzi TSSA variants and one TSSA sequence from the phylogenetically related bat parasite T. cruzi marinkellei. Further residue permutation analyses enabled the identification of diagnostically relevant or non-relevant substitutions among TSSA natural polymorphisms. Interestingly, T. cruzi marinkellei TSSA displayed specific serorecognition by one chronic Chagas disease patient from Colombia, which warrant further investigations on the diagnostic impact of such atypical TSSA. CONCLUSIONS/SIGNIFICANCE: Overall, our findings shed new light into TSSA evolution, epitope landscape and modes of recognition by Chagas disease patients; and have practical implications for the design and/or evaluation of T. cruzi serotyping strategies. Public Library of Science 2023-08-09 /pmc/articles/PMC10441789/ /pubmed/37556493 http://dx.doi.org/10.1371/journal.pntd.0011542 Text en © 2023 Romer et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Romer, Guadalupe
Bracco, Leonel A.
Ricci, Alejandro D.
Balouz, Virginia
Berná, Luisa
Villar, Juan C.
Ramsey, Janine M.
Nolan, Melissa S.
Torrico, Faustino
Kesper, Norival
Altcheh, Jaime
Robello, Carlos
Buscaglia, Carlos A.
Agüero, Fernán
Deep serological profiling of the Trypanosoma cruzi TSSA antigen reveals different epitopes and modes of recognition by Chagas disease patients
title Deep serological profiling of the Trypanosoma cruzi TSSA antigen reveals different epitopes and modes of recognition by Chagas disease patients
title_full Deep serological profiling of the Trypanosoma cruzi TSSA antigen reveals different epitopes and modes of recognition by Chagas disease patients
title_fullStr Deep serological profiling of the Trypanosoma cruzi TSSA antigen reveals different epitopes and modes of recognition by Chagas disease patients
title_full_unstemmed Deep serological profiling of the Trypanosoma cruzi TSSA antigen reveals different epitopes and modes of recognition by Chagas disease patients
title_short Deep serological profiling of the Trypanosoma cruzi TSSA antigen reveals different epitopes and modes of recognition by Chagas disease patients
title_sort deep serological profiling of the trypanosoma cruzi tssa antigen reveals different epitopes and modes of recognition by chagas disease patients
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10441789/
https://www.ncbi.nlm.nih.gov/pubmed/37556493
http://dx.doi.org/10.1371/journal.pntd.0011542
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